人-珠蛋白基因5'侧区可能的抑制元件分析。

J M Krakowsky, E S Panke, R F Lee, J McNeish, S S Potter, J B Lingrel
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引用次数: 5

摘要

人类β -珠蛋白基因的表达主要局限于成人,在胚胎或胎儿期很少或不表达该基因。该基因在胚胎和胎儿红系组织中缺乏表达可能是由于这些细胞中缺乏所需的正调节因子或存在阻止成人珠蛋白基因表达的负调节因子。为了测试抑制因子模型,我们使用了凝胶电泳迁移转移法来鉴定人类β -珠蛋白基因中与K562细胞中发现的蛋白质结合的区域,K562细胞表达胚胎和胎儿珠蛋白,但不表达成人β -珠蛋白。利用K562细胞的核蛋白分析了包含整个人类β -珠蛋白基因的DNA片段,发现了四个结合蛋白的区域。它们位于基因的5'侧区,第一和第二内含子内,以及3'侧区。先前的研究表明外显子2的潜在抑制位点5'的存在。出于这个原因,我们研究了5'侧序列中缺乏结合区域是否允许在胚胎期转基因小鼠中表达人-珠蛋白基因。β -珠蛋白基因的表达仅限于成人,这表明如果一个转录抑制因子在胚胎组织中负责使该基因失活,那么它并不仅仅受人类β -珠蛋白基因5'侧区- 122bp上游序列的调控。
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Analysis of possible repressor elements in the 5'-flanking region of the human beta-globin gene.

Human beta-globin gene expression is confined predominantly to the adult with little or no expression of this gene occurring during embryonic or fetal life. The lack of expression of this gene in embryonic and fetal erythroid tissue could be due to the absence of required positive regulatory factors in these cells or the presence of negative regulatory factors which prevent expression of the adult globin gene. To test the repressor model, we have used a gel electrophoretic mobility shift assay to identify regions in the human beta-globin gene which bind proteins found in K562 cells, a cell line that expresses embryonic and fetal globins but not adult beta-globin. DNA fragments comprising the entire human beta-globin gene were assayed using nuclear proteins from K562 cells, and four regions were found that bind proteins. These are located within the 5'-flanking region, within the first and second introns, and at the 3'-flanking region of the gene. Previous studies have suggested the presence of potential repressor sites 5' of exon 2. For this reason, we examined whether the lack of the binding regions in the 5'-flanking sequence allow expression of the human beta-globin gene in transgenic mice during embryonic life. beta-globin gene expression was confined to adult life, indicating that if a transcriptional repressor is responsible for inactivating this gene in embryonic tissue, it is not regulated solely by sequences upstream from -122 bp in the 5'-flanking region of the human beta-globin gene.

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